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通过体外重组鉴定,酿酒酵母动粒含有一种细胞周期蛋白 - CDK复合物同源物。

The Saccharomyces cerevisiae kinetochore contains a cyclin-CDK complexing homologue, as identified by in vitro reconstitution.

作者信息

Stemmann O, Lechner J

机构信息

Institut für Biochemie, Universität Regensburg, Germany.

出版信息

EMBO J. 1996 Jul 15;15(14):3611-20.

Abstract

We have developed methods to reconstitute the centromere DNA (CEN)-bound Saccharomyces cerevisiae kinetochore complex, CBF3, from isolated CBF3 components in vitro. This revealed that cooperation of at least three CBF3 components is imperatively required to form an activity that specifically binds to the centromere DNA in vitro. Two of the CBF3 proteins, Cbf3a and Cbf3b, that were used in the reconstitution were obtained from heterologous systems. In contrast, Cbf3c, the third CBF3 component known, had to be purified from S. cerevisiae to obtain a Cbf3c preparation that was competent to reconstitute the CBF3-CEN complex in combination with Cbf3a and Cbf3b. This led to the identification of a 29 kDa protein that co-purified with Cbf3c. The 29 kDa protein was shown to be a fourth component of CBF3 and therefore was named Cbf3d. Analysing the Cbf3d gene revealed that Cbf3d exhibits strong homology to p19SKP1, a human protein that is part of active cyclin A-CDK2 complexes. Therefore, Cbf3d is the only CBF3 protein that has a known homologue in higher eukaryotes and may provide the anchor that directs cell cycle-regulated proteins to the kinetochore.

摘要

我们已经开发出了从体外分离的CBF3组分中重建着丝粒DNA(CEN)结合的酿酒酵母动粒复合体CBF3的方法。这表明,体外形成一种能特异性结合着丝粒DNA的活性,至少需要三种CBF3组分协同作用。用于重建的两种CBF3蛋白Cbf3a和Cbf3b是从异源系统中获得的。相比之下,已知的第三种CBF3组分Cbf3c必须从酿酒酵母中纯化,才能获得一种能与Cbf3a和Cbf3b结合重建CBF3 - CEN复合体的Cbf3c制剂。这导致鉴定出一种与Cbf3c共纯化的29 kDa蛋白。该29 kDa蛋白被证明是CBF3的第四个组分,因此被命名为Cbf3d。对Cbf3d基因的分析表明,Cbf3d与p19SKP1具有很强的同源性,p19SKP1是一种人类蛋白,是活性细胞周期蛋白A - CDK2复合体的一部分。因此,Cbf3d是唯一在高等真核生物中有已知同源物的CBF3蛋白,可能提供将细胞周期调节蛋白导向动粒的锚定物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3cf/451974/f01bd4c7df78/emboj00014-0129-a.jpg

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